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Biochemistry of neurotransmitters
Dr. Mamoun AhramNeuroscience
2014
References
• This lecture• Mark’s Basic Medical Biochemistry, 4th ed, pp. 908-
918• http://what-when-how.com/neuroscience/
neurotransmitters-the-neuron-part-1/
What is a neurotransmitter?
• A chemical substance that:– Is synthesized and stored in a presynaptic neuron (the
enzymes needed for its synthesis must be present in the neuron),
– Is released at a synapse following depolarization of the nerve terminal (usually dependent on influx of calcium ions),
– binds to receptors on the postsynaptic cell and/or presynaptic terminal,
– elicits rapid-onset and rapidly reversible responses in the target cell,
– Is removed or inactivated from the synaptic cleft.
Types of neurotransmitters
• Small-molecule– Amines (acetylcholine, epinepherine, dopamine,
histmaine, etc.)– Amino acids (glutamate, aspartate)
• Neuropeptides• Gases (nitric oxide)
Note the differences
• Onset and duration of action• Concentration for action and receptor binding• Concentration of [Ca+] for release• Site of synthesis, modification• Fate
NEUROPEPTIDES
Introduction
• More than 50 neuropeptides have been described – Behavior– Pain perception– Memory– Appetite– Thirst– Temperature– Homeostasis– Sleep
Neuropeptides: neurohormones or neurotransmitters?• Neurohormones: when neurons secrete their
peptides into the vascular system to be transported to a relatively distant target
• Neurotransmitter: Many axon terminals of neurosecretory cells secrete their products at the synapse to directly affect a post synaptic cell
• Neuropeptides can do both – depends on nerve terminal
Stages of action
• Synthesis (ER and Golgi apparatus)
• Packaging into large-dense core vesicles (with modifying enzymes)
• Transport (fast-axonal transport)
• Release• Action (prolonged)• Termination by diffusion
and degradation
Synthesis is sequential
Synthesis is tissue-specific
Synthesis is controlled by alternative splicing
Role of calcium
Neuropeptides
• The endogenous opiates• Neuropeptide Y• Galanin• Pituitary adenylate cyclase–activating peptide (PACAP) • Melanocyte-stimulating hormone (MSH)• Neurokinin A (NKA)• Substance P (SP)• Neurotensin• Calcitonin-gene–related protein (CGRP)• Vasoactive intestinal polypeptide (VIP)
Substance P
• Member of tachykinins family • 11-amino acid peptide• Act via neurokinin receptors 1, 2, or 3 (GPCR) and Gs• Functions: vasodilation, inflammatory response, pain
perception• Pathological connection: eczema, fibromyalgia, GI
infection
Nerve growth factor (NGF)
• Member of the neurotrophin family• 118-acid polypeptide hormone• Act via tyrosine kinase receptors• Affect tissue immune reactivity
Neuropeptide Y
• A 36 amino acid peptide• Acts via G-protein coupled receptors (decrease in
cAMP, decrease in Ca+2 , and increase in K+ conductance)
• Function: augments the vasoconstrictor effects of norepinephrine
SMALL-MOLECULE NEUROTRANSMITTERS
Types of small-molecule neurotransmitter• Nitrogen-containing molecules – amino acids and their derivatives– intermediates of glycolysis and the Krebs cycle (TCA
cycle)
Stages of action
• Synthesis of enzymes– Cytosol– ER-Golgi apparatus (packaging
into large-dense core vesicles)• Transport of enzymes (slow and
fast-axonal transport)• Synthesis in pre-synaptic terminal• Packaging in synaptic vesicles• Release• Action (short)• Termination by diffusion, re-
uptake, or inactivation
[Ca = ]+2 mM
[Ca = ]+0.1 uM
[Ca = ]+50-100 uM
Synaptic vs. large dense core vesicles
Role of clathrin and dynamin
SPECIFIC EXAMPLES OF NEUROTRANSMITTER SYNTHESIS
But first, note
• Role of cofactors– S-adenosylmethionine (methyl transfer)– Pyrodoxal phosphate (vitamin B6): transamination,
decarboxylation– Tetrahydrobiopterin (BH4)
TYROSINE-DERIVED NEUROTRANSMITTERS
Dopamine, norepinephrine, and epinephrine
Rate-limiting step
Pyridoxal phosphate vesicular
Vitamin B12 or folate
Diet/liver
phenylalanine hydroxylase
50%
COMT and MAO
Parkinson’s disease
Regulation
• Tyrosine hydroxylase– Short term• Inhibition by free cytosolic catecholamines
• Catecholamines compete with BH4 binding to enzyme
• Activation by depolarization – Tight binding to BH4 following phosphorylation by PKA, CAM
kinases, PKC
– Long-term (plus dopamine -hyroxylase)
TRYPTOPHAN-DERIVED NEUROTRANSMITTERS
Serotonin and melatonin
BH4
Serotonin
5-hydroxyindoleacetic acid
urine
MAO
Antidepressants , called selective serotonin re-uptake inhibitors (SSRIs), like Prozac® inhibit the reuptake process resulting in prolonged serotonin presence in the synaptic cleft.
Melatonin
• Serotonin synthesized in the pineal gland serves as a precursor for the synthesis of melatonin, which is a neurohormone involved in regulating – sleep patterns– Seasonal and circadian (daily) rythyms– Dark-light cycle
GLUTAMATE AND ASPARTATE
Glutamate and aspartate
• Nonessential amino acids • Do not cross BBB – must be synthesized in neurons
• Main synthetic compartments– neurons – glial cells
• Both are excitatory neurotransmitters.
GABA
glutaminaseGlutaminesynthetase
transaminase1
2
3
-KG
GluDehydro
• Two pathways:• Glycolysis Krebs cycle
Transamination or dehydrogenation
• Glutamine (deamination)• Another source: aspartate• Removal
– excitatory amino acid carrier-1 (EAAC1)
– glutamate transporter-1 (GLT-1) and glutamate—aspartate transporter (GLAST)
Synthesis of glutamate
Sources of glutamate (supplementary)
Physiological and clinical implications• Excitatory amino acids may be involved in learning and
memory processes, as well as motor functions.• Chronic neuropathological conditions such as amyotrophic
lateral sclerosis [ALS] (also known as Lou Gehrig’s disease).– degeneration of the motor neurons in the anterior horn of
the spinal cord, brainstem, and cerebral cortex.• Prolonged stimulation of neurons by excitatory amino acids
results in neuronal death or injury.• Overexcitatory effects result in Alzheimer’s disease.
Aspartate
• A vesicular uptake mechanism for aspartate has not yet been demonstrated, somewhat weakening the case for considering aspartate to be a neurotransmitter
• Precursor: oxaloacetate (transmamination)
Glycine
• The major inhibitory neurotransmitter in the spical cord
• Synthesized from serine by serine hydroxymethyltransferase through 3-phosphoglycerate
• Removal: high-affinity transporter
OTHERS
GABA
• GABA is present in high concentrations (millimolar) in many brain regions. – These concentrations are about 1,000 times higher
than concentrations of the classical monoamine neurotransmitters in the same regions.
• The GABA shunt is a closed-loop process with the dual purpose of producing and conserving the supply of GABA.
GABA shunt
Diet
MembranePL
Synthesis of acetylcholine
• Choline + acetylcoenzyme-A by choline acetyltransferase in cytoplasm
• Transported into and stored in vesicles.
• Removal: hydrolysis by acetylcholinesterase
Histamine
• it does not penetrate the blood—brain barrier and, hence, must be synthesized.
Pyridoxal phosphate
AstrocytesNeuron
X
Inactivation of histamine
Nitric oxide (NO)
• Glutamate is released (1) and acts on NMDA receptors located on the post-synaptic neuron (2)
• Ca2+ enters the postsynaptic neuron and binds with calmodulin activating NOS (3) resulting in formation of NO and citrulline from L-arginine (4).
• No stimulates guanylate cyclase forming cGMP (5), which results in a physiological response (6)
• No can diffuse out: a) to the presynaptic terminal (7) prolonging effect and b) into adjacent neurons (8) and glial cells (9) stimulating guanylate cyclase
Is NO a neurotransmitter?
• Yes, but:– It is not stored in vesicles– It is not released by calcium-dependent exocytosis (it diffuses)– Its inactivation is passive (there is no active process that
terminates its action)• It decays spontaneously
– It does not interact with receptors on target cells• Its sphere of action depends on the extent to which it diffuses,
and its action is not confined to the conventional presynaptic-postsynaptic direction.
– NO acts as a retrograde messenger and regulates the function of axon terminals presynaptic to the neuron in which it is synthesized.
Nitric oxide (NO)
• Half-life: 2-4 seconds
• NO is inhibited by hemoglobin and other heme proteins which bind it tightly
NO synthase
• Isoform I (nNOS or cNOS)– Neurons and epithelial cells– activated by the influx of extracellular calcium
• isoform II (iNOS)– Macrophages and smooth muscle cells – induced by cytokines
• and isoform III (eNOS)– Endothelial cells lining blood vessels – activated by the influx of extracellular calcium
• All three isoforms require BH2 as a cofactor and nicotinamide adenine dinucleotide phosphate (NADPH) as a coenzyme
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